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系统给予 8-OH-DPAT 和 eticlopride,但不是 SCH23390,会改变大鼠的追失行为。

Systemic administration of 8-OH-DPAT and eticlopride, but not SCH23390, alters loss-chasing behavior in the rat.

机构信息

Department of Psychiatry, University of Oxford, Oxford, UK.

出版信息

Neuropsychopharmacology. 2013 May;38(6):1094-104. doi: 10.1038/npp.2013.8. Epub 2013 Jan 7.

DOI:10.1038/npp.2013.8
PMID:23303072
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3629409/
Abstract

Gambling to recover losses is a common gaming behavior. In a clinical context, however, this phenomenon mediates the relationship between diminished control over gambling and the adverse socioeconomic consequences of gambling problems. Modeling loss-chasing through analogous behaviors in rats could facilitate its pharmacological investigation as a potential therapeutic target. Here, rats were trained to make operant responses that produced both food rewards, and unpredictably, imminent time-out periods in which rewards would be unavailable. At these decision points, rats were offered choices between waiting for these time-out periods to elapse before resuming responding for rewards ('quit' responses), or selecting risky options with a 0.5 probability of avoiding the time-outs altogether and a 0.5 probability of time-out periods twice as long as signaled originally ('chase' responses). Chasing behavior, and the latencies to chase or quit, during sequences of unfavorable outcomes were tested following systemic administration of the 5-HT1A receptor agonist, 8-OH-DPAT, the D2 receptor antagonist, eticlopride, and the D1 receptor antagonist, SCH23390. 8-OH-DPAT and eticlopride significantly reduced the proportion of chase responses, and the mean number of consecutive chase responses, in a dose-dependent manner. 8-OH-DPAT also increased latencies to chase. Increasing doses of eticlopride first speeded, then slowed, latencies to quit while SCH23390 had no significant effects on any measure. Research is needed to identify the precise cognitive mechanisms mediating these kinds of risky choices in rats. However, our data provide the first experimental demonstration that 5-HT1A and D2, but not D1, receptor activity influence a behavioral analog of loss-chasing in rats.

摘要

赌博以挽回损失是一种常见的赌博行为。然而,在临床环境中,这种现象调节了赌博控制能力下降与赌博问题的不良社会经济后果之间的关系。通过大鼠中类似行为对追损失现象进行建模,可以促进对其作为潜在治疗靶点的药理学研究。在这里,大鼠被训练做出操作性反应,这些反应既能产生食物奖励,又能不可预测地立即进入无奖励的时间限制期。在这些决策点上,大鼠可以选择等待时间限制期过去,然后恢复获得奖励的反应(“放弃”反应),或者选择有 0.5 概率完全避免时间限制期和 0.5 概率时间限制期延长为原来信号的两倍的风险选项(“追逐”反应)。在系统给予 5-HT1A 受体激动剂 8-OH-DPAT、D2 受体拮抗剂 eticlopride 和 D1 受体拮抗剂 SCH23390 后,测试了不利结果序列中追逐行为以及追逐或放弃的潜伏期。8-OH-DPAT 和 eticlopride 以剂量依赖性方式显著降低了追逐反应的比例和连续追逐反应的平均数量。8-OH-DPAT 还增加了追逐的潜伏期。递增剂量的 eticlopride 首先加速,然后减慢,放弃的潜伏期,而 SCH23390 对任何测量都没有显著影响。需要研究来确定介导大鼠这种风险选择的精确认知机制。然而,我们的数据首次提供了实验证据,表明 5-HT1A 和 D2,但不是 D1,受体活性会影响大鼠行为类似的追损失现象。

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